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Combinatorial transcriptional control in blood stem/progenitor cells: genome-wide analysis of ten major transcriptional regulators.

机译:血液干/祖细胞中的组合转录控制:十种主要转录调节因子的全基因组分析。

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摘要

Combinatorial transcription factor (TF) interactions control cellular phenotypes and, therefore, underpin stem cell formation, maintenance, and differentiation. Here, we report the genome-wide binding patterns and combinatorial interactions for ten key regulators of blood stem/progenitor cells (SCL/TAL1, LYL1, LMO2, GATA2, RUNX1, MEIS1, PU.1, ERG, FLI-1, and GFI1B), thus providing the most comprehensive TF data set for any adult stem/progenitor cell type to date. Genome-wide computational analysis of complex binding patterns, followed by functional validation, revealed the following: first, a previously unrecognized combinatorial interaction between a heptad of TFs (SCL, LYL1, LMO2, GATA2, RUNX1, ERG, and FLI-1). Second, we implicate direct protein-protein interactions between four key regulators (RUNX1, GATA2, SCL, and ERG) in stabilizing complex binding to DNA. Third, Runx1(+/-)::Gata2(+/-) compound heterozygous mice are not viable with severe hematopoietic defects at midgestation. Taken together, this study demonstrates the power of genome-wide analysis in generating novel functional insights into the transcriptional control of stem and progenitor cells.
机译:组合转录因子(TF)相互作用控制细胞表型,并因此支持干细胞的形成,维持和分化。在这里,我们报告了全基因组结合模式和血液干细胞/祖细胞的十个关键调控因子(SCL / TAL1,LYL1,LMO2,GATA2,RUNX1,MEIS1,PU.1,ERG,FLI-1和GFI1B)的组合相互作用),从而为迄今为止的任何成体干/祖细胞类型提供最全面的TF数据集。全基因组的复杂结合模式的计算分析,然后进行功能验证,揭示了以下内容:首先,七种TF(SCL,LYL1,LMO2,GATA2,RUNX1,ERG和FLI-1)之间以前无法识别的组合相互作用。其次,我们暗示了四个关键调节因子(RUNX1,GATA2,SCL和ERG)之间的直接蛋白质-蛋白质相互作用,以稳定复合物与DNA的结合。第三,Runx1(+/-):: Gata2(+/-)复合杂合小鼠在妊娠中期不具有严重的造血缺陷。两者合计,这项研究证明了全基因组分析的力量在产生对干细胞和祖细胞转录控制的新颖功能见解中。

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